The flounder organic anion transporter fOat has sequence, function, and substrate specificity similarity to both mammalian Oat1 and Oat3

doi:10.1152/ajpregu.00326.2006

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Am J Physiol Regul Integr Comp Physiol 291: R1773-R1780, 2006. First published July 20, 2006; doi:10.1152/ajpregu.00326.2006
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COMPARATIVE AND EVOLUTIONARY PHYSIOLOGY

The flounder organic anion transporter fOat has sequence, function, and substrate specificity similarity to both mammalian Oat1 and Oat3

Amy G. Aslamkhan,¹^,2^,* Deborah M. Thompson,¹^,* Jennifer L. Perry,¹ Kelly Bleasby,¹ Natascha A. Wolff,³ Scott Barros,¹ David S. Miller,¹^,2 and John B. Pritchard¹

¹Laboratory of Pharmacology and Chemistry, National Institute of Environmental Health Sciences, Research Triangle Park, North Carolina; ²Mount Desert Island Biological Laboratory, Salisbury Cove, Maine; and ³Zentrum Physiologie und Pathophysiologie, Abteilung Vegetative Physiologie und Pathophysiologie, Göttingen, Germany

Submitted 15 May 2006 ; accepted in final form 7 July 2006

The flounder renal organic anion transporter (fOat) has substantialsequence homology to mammalian basolateral organic anion transporterorthologs (OAT1/Oat1 and OAT3/Oat3), suggesting that fOat mayhave functional properties of both mammalian forms. We thereforecompared uptake of various substrates by rat Oat1 and Oat3 andhuman OAT1 and OAT3 with the fOat clone expressed in Xenopusoocytes. These data confirm that estrone sulfate is an excellentsubstrate for mammalian OAT3/Oat3 transporters but not for OAT1/Oat1transporters. In contrast, 2,4-dichlorophenoxyacetic acid andadefovir are better transported by mammalian OAT1/Oat1 thanby the OAT3/Oat3 clones. All three substrates were well transportedby fOat-expressing Xenopus oocytes. fOat K_m values were comparableto those obtained for mammalian OAT/Oat1/3 clones. We also characterizedthe ability of these substrates to inhibit uptake of the fluorescentsubstrate fluorescein in intact teleost proximal tubules isolatedfrom the winter flounder (Pseudopleuronectes americanus) andkillifish (Fundulus heteroclitus). The rank order of the IC₅₀values for inhibition of cellular fluorescein accumulation wassimilar to that for the K_m values obtained in fOat-expressingoocytes, suggesting that fOat may be the primary teleost renalbasolateral Oat. Assessment of the zebrafish (Danio rerio) genomeindicated the presence of a single Oat (zfOat) with similarityto both mammalian OAT1/Oat1 and OAT3/Oat3. The puffer fish (Takifugurubripes) also has an Oat (pfOat) similar to mammalian OAT1/Oat1and OAT3/Oat3 members. Furthermore, phylogenetic analyses arguethat the teleost Oat1/3-like genes diverged from a common ancestralgene in advance of the divergence of the mammalian OAT1/Oat1,OAT3/Oat3, and, possibly, Oat6 genes.

OAT1; OAT3; renal; isolated tubules

Address for reprint requests and other correspondence: J. B. Pritchard, National Institute of Environmental Health Sciences, Laboratory of Pharmacology and Chemistry, PO Box 12233, F1-03, Research Triangle Park, NC 27709 (e-mail: pritcha3{at}niehs.nih.gov)

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